JPH06508840A - Dibenzo[b,e]azepine derivatives and pharmaceutical compositions containing the same - Google Patents

Abstract

(57) [Summary] This bulletin contains application data before electronic filing, so abstract data is not recorded.

Description

[Detailed description of the invention] Dibenzo(b,e)azepine derivatives and pharmaceutical compositions containing the same The subject matter of the present invention is dibenzo[b,e]azepine derivatives, their preparation process and their In a pharmaceutical composition containing the compound.

The present invention is based on the general formula ■; [Wherein A is methylene, carbonyl, thiocarbonyl, carbimino, N-hydro represents a oxy-rubimino or sulfonyl group, where X is a valence bond, oxygen or sulfur group; child, sulfinyl or sulfonyl group, CH25 group or NH group, and n is Represents an integer from 1 to 3, and R1 to R' are independently the same or different. hydrogen atoms, straight chain or branched chains having 1 to 6 carbon atoms, or saturated or is an unsaturated aliphatic group, C, -C, alkoxy, CI-C, alkylmercapto, C , -C, alkylsulfinyl, C, -C, alkylsulfonyl, amino, C, -C, alkylamino, diC, -C, alkylamino, sulfonamide, Cl- C6 alkoxycarponyl, carboxyl, halogen, hydroxyl, nitro, represents cyano, azide, phenyl or benzyloxy, and R4 is hydrogen, or or a linear or branched saturated or unsaturated aliphatic group having 1 to 6 carbon atoms. ] Dibenzo [b, e) azepine derivatives, their tautomers, enantiomers , diastereomers and physiologically compatible salts.

The research underlying the present invention can utilize novel dibenzo(b,e]azepine derivatives. It was to be done. These compounds are used in particular for the preparation of medicaments.

The compounds of the invention exhibit beneficial pharmacological effects. Among other things, they are DNA viruses, For example, herpes simplex virus, cytomegalovirus, papillomavirus, varicella-zoster Herpes virus or Epstein-Barr virus, or RNA virus, e.g. Batogaviruses, especially retroviruses, such as tumor viruses HTLV-I and ■, and lentivirus Visna and human immunodeficiency virus HIV-1 and It is suitable for the treatment and prevention of infectious diseases caused by -2.

Compounds of formula I are useful in clinical manifestations of retroviral HIV infection in humans, e.g. Persistent generalized lymphadenopathy (PGL), advanced stage AIDS-related syndrome (ARC) and appears to be particularly suitable for treating clinically complete AIDS symptoms.

The compound of general formula (■) according to the present invention has a remarkable antiviral effect, especially against viruses. It is suitable for the treatment of viral and retroviral infections. mammals, especially humans, Viral infections are widespread throughout the world. Despite intensive efforts, until now The appearance of a disease caused by a virus or retrovirus, either causally or symptomatically Interfering chemotherapy has not had appreciable success. Some kind of virus today diseases, such as acquired immunodeficiency syndrome (AIDS), AIDS-related syndromes (ARC) and its preliminary stages, herpes, cytomegalovirus (CMV), influenza and other viral infections, and chemotherapy is effective in treating these conditions. cannot influence it. Currently, for example, in the treatment of AIDS, Topsin (zidovudine) or Retrovir (Retrovir■) and The most common is 3゛-azido-3'-deoxythymidine (AZT), which is known as It is used exclusively. However, AZT has a very broad therapeutic spectrum. Characterized by narrowness or extreme toxicity already present in the therapeutic range. (Hirsch.

M, S, (1988) J, 1nfec, Dis, 157.427-4 31). Compounds of general formula I do not have these drawbacks. They are pharmacologically It acts antivirally without being cytotoxic at relevant doses.

Here, compounds of general formula I have been shown to induce D It was found to inhibit the growth of NA and RNA viruses. these substances can affect retrovirus growth by inhibiting reverse transcriptase ( Proc, Natl.

Eliminate diseases caused by retroviruses without affecting normal natural body functions. There is a great need for chemotherapy that blocks as specifically as possible The compounds listed above may be associated with retroviral infections pathophysiologically, symptomatically, or clinically. may be of advantageous prophylactic or therapeutic use in the treatment of related diseases. .

Separation of racemic compounds into enantiomers can be achieved using a suitable optically active phase using conventional eluents. to be carried out analytically, semi-preparatively, or preparatively by chromatography at Can be done.

As optically active phase, for example optically active polyacrylamide or polymethane Acrylamide, partially supported on silica gel [e.g., Merck ChiraSpher■, Baker's chiral pack ( Chiralpak ■) 0T10P), cellulose ester/carbamide [For example, Chiracel ■ manufactured by Baker/Daice1] 0B10Y), a phase based on cyclodextrin or crown ether [ For example, Daice1's Crownpak ■ or micro Examples include crystalline cellulose triacetate (manufactured by Merck).

In the general formula I, A represents in particular a methylene, carbonyl or thiocarbonyl group. However, the carbonyl group is particularly problematic.

X especially represents an oxygen or sulfur atom or a sulfinyl or sulfonyl group .

n preferably represents the number 1 or 2.

For groups R1 to R3, hydrogen, C, -C, alkyl, C2-C, alkenyl, C, -C, alkynyl, C1-C5 alkoxy, C, -C, alkylmercapto , C, -CM alkylamino, C1-C5 alkoxycarbonyl, amino, halo Gen, hydroxyl, cyano and azide are preferred. Science is 7-18-19- Alternatively, the 10-position may be substituted with R1, with the 8- and 9-positions being preferred.

R1 particularly represents a halogen atom or a C, -C, alkyl group.

Substituents R2 and R3 may be present at the 1-12-13- or 4-positions of the 3- and 4-positions are preferred. R2 especially represents a hydrogen atom and R3 Hydrogen atom, halogen atom, C, -C, alkyl or CtCs alkoxy group represent. In this sense, R1 is in particular a chlorine atom, a methyl or a methoxy group. .

For the group R4, hydrogen, C, -C, alkyl, C2C<alkenyl and C2 -C4 alkynyl is preferred.

For the radicals R'-R3, independently of each other hydrogen, methyl, ethyl, isopropyl allyl, methoxy, ethoxy, methylmercapto, ethylmercaptomethyl Amino, methoxycarbonyl, ethoxycarbonyl, amino, azide, cyano, Hydroxyl and halogen are particularly preferred, with halogen being preferably chlorine and bromine. Yes. For R4, hydrogen, methyl, ethyl, isopropyl and allyl are particularly preferred. preferred.

The aliphatic group in the definition of R1 is a linear or branched saturated or unsaturated group. all containing up to 6 carbon atoms.

As saturated groups, C, -C, alkyl groups, such as methyl, ethyl, n-propyl, Problems include i-propyl, n-butyl, i-butyl or t-butyl. unsaturated The groups are especially CtCa alkenyl and C2-C,alkynyl groups, which are branched and for example allyl, vinyl, 2-butenyl or propargyl.

Pharmaceutical compositions containing at least one compound of formula I for treating viral infections The composition can be administered enterally or parenterally in liquid or solid form. . In that case, for example, tablets, capsules, dragees, syrups, solutions or Common dosage forms such as suspensions are problematic. As an injection medium, preferably a safe Water containing additives commonly used in injection solutions, such as fixing agents, solubilizing agents, and buffering agents, is used. I can stay. Such additives include, for example, tartaric acid and citrate buffers, ethanol , complexing agents such as ethylenediaminetetraacetic acid and its non-toxic salts, for viscosity adjustment High molecular weight polymers such as liquid polyethylene oxide. Liquid carrier for injections The body material must be sterile and preferably filled into ampoules. solid carrier Body substances include, for example, starch, lactose, mannitol, methylcellulose, and luc, highly dispersed silicic acid, high molecular weight fatty acids (e.g. stearic acid), gelatin, agar, High in calcium phosphate, magnesium stearate, animal and vegetable fats, solids molecular polymers (eg polyethylene glycol) and the like. Suitable for oral administration The composition may optionally include flavoring or sweetening substances.

Physiologically compatible salts include inorganic or organic acids, such as halogen acids (HCI, HB). r, etc.), acid addition salts with sulfuric acid, phosphoric acid, tartaric acid, succinic acid, oxalic acid, acetic acid, etc. It is.

Dosage depends on a variety of factors, including method of administration, species, age, and individual health status. . The compounds of the invention are usually administered at 0.1-100 mg/kg body weight/day, preferably is administered in an amount of 0.2 to 80 mg/day. Divide the daily dose into 2 to 5 doses. , administering 1 to 2 tablets each time with an active substance content of 0.5 to 500 mg. is preferable. Tablets can also be extended-release, in which case the number of doses per day is reduced to 1. Reduce to ~3 times. The active substance content of sustained release tablets can be from 2 to 1000 mg. Ma Alternatively, the active substance may be administered by continuous infusion, usually in doses of 5 to 50 mg per day. An amount of looOmg is sufficient.

The compounds of general formula I according to the invention are prepared by methods known per se, which include a) Formula 11: [In the formula, A, X, n and R'-R' have the above meanings, and Y represents a reactive group. or b) a compound of formula III: A compound of [wherein A, X, n, R'=R' and Y have the above meanings] , with separation of HY; or C) formula ■v: A compound of the formula V in which A, X and R'-R' have the above meanings: y' - (CH2), -Y' (V) [wherein n has the above meaning, and Y' and Y' are the same or different, Y with the meaning of ] with the separation of HY' and HY'. or d) Formula V1: [wherein A, X, n and R'-R' have the above meanings, and Z is a reactive or e) one or more of the n CHt groups; By reduction, a compound of formula (1) in which more than one is substituted with CO or a derivative thereof Convert to a compound of formula ■; And, as the case may be, the compound of the formula (III) may be converted into another compound of the formula (I) within the scope of the claims. titration with a pharmacologically compatible acid or base, if desired. It consists of converting it into salt. Racemic compounds are, for example, cellulose Separation into enantiomers by chromatography on a suitable optically active phase such as acetate can be released.

As reactive groups X, Y, Y' and Y', easily cleavable groups, especially The halogen atoms, mesyloxy and tosyloxy groups become a problem. HYSHY ’ and HY’ can be conveniently separated in a solvent in the presence of a base, e.g. Alkali metal alcolade in solution, potassium carbonate in acetone or butanone , in toluene or dimethylformamide in the presence of sodium hydride.

Regarding the reactive group Z, in addition to those listed for Y, lower alkoxy groups, Also included are optionally substituted phenoxy or azido groups.

For convenience, reduction of carbonyl group to CH2 group is carried out using lithium aluminum hydride or boron. Hydrogen activated by double metal hydrides, such as sodium hydride, or by catalysts This is done using

The starting materials of formulas II to vI are known from the literature or are known from known materials. It can be manufactured according to the method of

In the spirit of the present invention, the compounds described in the examples and the components described in the claims are In addition to those by combination of all meanings of substituents, racemic mixtures or optical A compound of the following formula ■ existing in the active form or as the R- and S-enantiomers is It becomes a problem.

1.5.6-Sihydro11.5-thiomethano-11'H-dibenzo (b,e) Thiazepine 6-one; 2.1-Methyl-5,6-sihydro-11,5-thioethano-IIH-dibenzo [b, e) Azepin-6-one; 3,2-methyl-5,6-sihydro 11.5 -thioethano-1LH-dibenzo[b,e]thiazepine 6-one; 4,3-methy -5,6-dihydro-11.5-thioethano-1LH-dibenzo[b,e) Zepin-6-one; 5,4-methyl-5,6-sihydro-11,5-thioethano -1IH-dibenzo(b,e)azepin-6-one; 6,3-chloro-5,6- sihydro11,5-thioethano-1IH-dibenzo(b,e]thiazepine 6- 7,4-chloro-5,6-cyhydro11,5-thioethano-IIH-di Benzo(b,e)thiazepine 6-one; 8,3-methoxy-5,6-sihydro 11.5-thioethano-11H-dibenzo[b,e]thiazepin 6-one; 9. 4-Methoxy-5,6-sihydro-11.5-thioethano-11H-dibenzo[ b, el azepin-6-one; 10.8-chloro-5,6-sihydro 11,5 -thioethano-1IH-dibenzo[b,e]thiazepine 6-one; 11, 9- Chloro-5,6-sihydro11.5-thioethano-1IH-dibenzoCb,e ]Azepin-6-one; 12.9-methyl-5,6-dihydro-11,5-thio Ethano-11H-dibenzo[b,e) azepin-6-one; 13.9-methoxy -5,6-sihydro11.5-thioethano-1LH-dibenzo(b,elase Pin-6-on; 14, 5. 6-Sihydro11.5-thioethano-1LH -dibenzo[b,e) azepine; 15.6-gomi2-5,6-sihydro11.5-thioethano-11H-diben zo(b,e)thiazepine 16.6-oximino-5,6-dihydro-11,5-thioethano-1IH-di Benzo [b, el azepine; +7. 5. 6-sihydro-11,5-thioeta No-11H-dibenzo[b,e) azepine-6-thione; 18.6.11-dihydro-11,6-thionitanodibenzo (c.

f) [1,2) Thiazepine 5,5-dioxide; 19.11-methyl-5,6 -Sihydro11.5-thioethano-11H-dibenzo[b,e]thiazepine 6 -On; 20, 5. 6-Sihydro-5,11-propano-11H-dibenzo [b, e) azepin-6-one; 21, 5. 6-Sihydro II, 5-epoxyethano-11H-dibenzo[ b, e) Azepin-6-one: 22, 5. 6-Shihydro 11,5-imino Ethano-11H-dibenzoTo,e]azepin-6-one; 23, 5. 6-Sihydro5,11-ethano-118-dibenzo[b,el azepin-6-one; 24, 5. 6-Sihydro-11.5-thiopropano-11H-dibenzo[b , e) azepin-6-one; 25, 5. 6-sihydro11.5-methanothioethano-11H-dibenzo [b, e] Thiazepine 6-one; 26, 5. 6-sihydro11.5-thio Ethano-11H-dibenzo[b,el azepin-6-one 12-year-old xyto;2 7, 5. 6-Sihydro-11.5-thioethano-11H-dibenzo[b,e ) Azepin-6-one 12.12-dioxide.

50% sodium hydride in 20 ml of N,N-dimethylformamide (DMF) (White oil dispersion) Dissolved in a suspension of 240 mg in DMFloml 1l-(2-chloroethylthio)-5,6-sihydro118-dibenzo[b, e) Add a solution of 1.5 g (5 mmol) of azepin-6-one dropwise at 70°C, Stir for 1 h at 0 °C, evaporate, take up in dichloromethane, wash with water, dry, Evaporate and chromatograph on silica gel RP 18 (Merck) Refined by fee. Elute with methanol/water/acetic acid 40:60:1 and triturated with ether to give 680 mg of the title compound with a melting point of 201-202°C. (51% of theory) is obtained.

1l-(2-chloroethylthio)-5゜6-sihydro1 used as starting material 1H-dibenzo[b,e) azepin-6-one can be obtained as follows. Ru: a) 11-chloro-5,6-sihydro-11H-dibenzo (b.

e] Thiazepine 6-one (J, Pharm, Pharmakol, 21. 520 (1969)) 8. 0 g (33 mmol), dichloromethane 7 A mixture of 5 ml and 2.6 g (33 mmol) of mercaptoethanol was Stir at room temperature for 4 hours. Evaporated under vacuum, 1l-(2 -hydroxyethylthio)-5,6-dihydro 11H-dibenzo[b,e]a Zepin-6-one (9.5 g of oil, quantitative) is further reacted.

b) Crude product 14 above. 2 g (50 mmo I), dichloromethane A mixture of 70 ml and 5.5 ml of thionyl chloride is heated under reflux for 2 hours. . This is evaporated, triturated finely with ether and filtered. Melting point 170-17 1l-(2-chloroethylthio)-5,6-dihydro-11H-dibenzo at 2°C [b, e) 13.8 g (91% of theory) of azepin-6-one remain.

Example 2 5.6-Sihydro11.5-thioethano-118-dibenzo[b,e) azepi N-61 on 11-Mercapto-5,6-dihydro-0-11H-dihydride dissolved in 20 ml of DMF. 1,2- to a solution of benzo(b,e)azepin-6-one, 2 g (5 mmol) 0.43 ml (5 mmol) of dibromoethane was added dropwise, stirred at room temperature for 30 minutes, Heat to 70 °C and add 0.48 g of 50% sodium hydride in 20 ml of DMF. Drop a suspension of After stirring for 1 hour, evaporate, take up in dichloromethane, and add water. Wash, dry, evaporate and purify as described in Example 1.

420 mg (31% of theory) of the title compound are obtained, melting point 196-198°C.

11-Mercapto-5,6-sihydro 11H-dibenzo [b.

e] Azepin-6-one can be obtained as follows = 11-chloro-5 ,6-sihydro-11H-dibenzo (b.

e]Azepin-6-one 7, 2 g (30 mmol), thiourea 2゜7 A mixture of g and 60 ml of ethanol is heated at reflux under nitrogen for 6 hours.

Subsequently, 18 ml of 5N sei soda solution was added to this, and the mixture was heated under reflux for 2 hours. Acidified with hydrochloric acid, evaporated, taken up in water, extracted with dichloromethane, dried and and evaporate.

After finely trituring the residue with ether, an 11-metal solution with a melting point of 188-190°C Lucapto-5,6-sihydro-11H-dibenzo[b,e]azepin-6-one 4.5 g (62% of theory) are obtained.

Example 3 rac-5,6-dihydro-0-11.5-thioethano-118-dibenzo (b,e ) Racemic compound 30 for enantiomeric separation of azepin-6-one vs. Dissolve 0 mg in 30 ml of methanol, and prepare a particle sample with an inner diameter of 50 mm and a length of 300 mm. Merc k 16326) and 80% aqueous methanol (flow rate 7.5 ml/min, approx. 1. 5 bar).

After evaporation of the appropriate fractions and fine trituration with isohexane, the following compounds I got: a) From fraction 1: (-)-5,8-dihydro-11,5-thioethano-11H- Dibenzo[b,e]azepin-6-one, melting point 177-178°C, [α]. − 121'b) From fraction 2: (+)-5,e-dihydro-11,5-thioeta No-118-dibenzo(b,e) azepin-6-one, melting point 178-179°C, [α]o +117°5.6-sihydro11.5-thioethano-11H-dibe 1.4 g of the compound of Example 1 in 20 ml of 1,2-dimethoxyethane ( Add 2.6 g of aluminum chloride to a 5 mmol solution at room temperature and stir for 30 minutes. After stirring, 0.74 g of sodium borohydride is introduced within 1 hour. Stir for 3 hours After stirring, decompose with ice water, make alkaline, extract with dichloromethane, and dissolve into silica. Purify on gel. After elution with isohexane:ethyl acetate 3:l, the target compound 0 ．． 5 g (40% of theory) were obtained, melting point 220~ using ethereal hydrogen chloride solution. Convert to hydrochloride at 222°C.

Example 5 5.6-Sihydro-11,5-thioethano-118-dibenzo[b,e]azepi tion 2.1 g (7.9 mmol) of the compound of Example 1, 60 ml of toluene and La A mixture of 1.5 g of Wesson's reagent was heated under reflux for 6 hours, and an additional 1.5 g of Mix with Lawesson's reagent, heat again under reflux for 6 hours, and after evaporation, silicage Refine with a filtrate. After elution with isohexanecoethyl acetate 3:1, the title compound was obtained with 0.0% of the title compound. 6 g (27% of theory) are isolated. Melting point 1 after finely grinding with ether 92-193°C.

Example 6 5.6-Sihydro11.5-thiopropano-118-dibenzo(b,e)aze pin-6-on In a manner analogous to that described in Example 1, 1l-(3-chloropropylthio) -5,6-sihydro118-dibenzo[b.

e] Table of melting points 222-224°C from azepin-6-one and sodium hydride The title compound is obtained in 23% yield.

The above starting materials can be obtained as follows: a) 11-rioo-5,6 -Sihydro-11H-dibenzo (b.

e] Azepin-6-one 14.6 g (60 mmol), dichloro.

200 ml of methane and 3-mercaptopropionic acid5. 4m1 (60mmo The mixture in 1) was stirred at room temperature for 4 hours, extracted with soda solution, and the extract was acidified. and filter the product.

3-(5,6-sihydro-11H-dibenzo(b,e) with melting point 185-187°C azepin-6-one-11-yl)-mercaptopropionic acid 15.9 g (theoretical) 85% of the amount) is isolated.

b) 2.66 g of lithium aluminum hydride in 75 ml of tetrahydrofuran of the above acid in 125 ml of tetrahydrofuran. 6g (5 A solution of 0 mmo I) was added dropwise, heated under reflux for 5 hours, and decomposed with a normal salt solution. , extracted with ethyl acetate and purified on silica gel. Isohexane: ethyl acetate After elution with 3:l of 1l-(3-hydroxypropylene) with a melting point of 113-135°C, (b, e) azepin-6-one 8.1 g (54% of theory) are obtained.

C) Prepare the above intermediate and nitrogen chloride in a manner analogous to that described in Example 1b. 1 l-(3 -chloropropylthio)-5,6-sihydro1LH-dibenzo[b,e)aze Get pin-6-on.

5.6-Sihydro11.5-thioethano-11H-dibenzo[b,e]azepi 6-one 12-oxide Compound of Example 1 1. 3 g (5 mmo 1 ), a solution of 50 ml of acetone and 1.2 ml of 30% hydrogen peroxide at 50°C. Stir for an hour, mix with water and extract with ethyl acetate. Evaporate the extract into ether After finely grinding with 53% of the amount) is obtained as monohydrate.

Example 8 5.6-Sihydro11.5-thioethano-11H-dibenzo(b,e)azepi 6-one 12.12-dioxide compound of Example 1 in 30 ml of chloroform A solution of 1.3 g (5 mmol) of the compound was added to 3-chloropetrope in 30 ml of chloroform. Mixed with a solution of 2.1 g of hydrogen carbonate, stirred at room temperature for 1 hour, and dissolved in sodium hydrogen carbonate. solution and evaporate the organic phase. After finely grinding with ether, 0.9 g (60% of theory) of the title compound with a melting point of 244 DEG-246 DEG C. are obtained.

Example 9 Improvement of reverse transcriptase (RT) by dibenzo [b, e) azepine derivatives The test system uses purified RT from HIV-1 (expressed in E. coli using genetic engineering techniques). components of the initiation complex, e.g. adjacent primer binding sites as a template. In vitro transcript of HIV-LTR with It contains an 18mar oligonucleotide complementary to the primer binding site described above.

Recover [3H]-thymidine-5'-triphosphate by counting with a β-counter. Measure the inclusion [7]. ICs of the compounds tested in the table below. Show value. This value is the opposite Corresponds to the concentration of test substance that results in 50% inhibition of the transcriptase.

Copy and translation of written amendment) Submission form (Patent Law Article 184-8) January 5, 1994

Claims (6)

[Claims] 1. Formula I: ▲There are mathematical formulas, chemical formulas, tables, etc.▼(I) [In the formula, A is methylene, carbonyl, thiocarbonyl, carbimino, N-hydroxycarbimino or sulfonyl group where X is a valence bond, oxygen or sulfur atom, sulfinyl or sulfonyl group , represents a CH2S group or an NH group, n represents an integer of 1 to 3, and R1 to R3 are mutually may be independently the same or different, and hydrogen atoms and carbon atoms, respectively. Straight or branched chain saturated or unsaturated aliphatic group of number 1 to 6, C1-C6 alkyl xy, C1-C6 alkylmercapto, C1-C6 alkylsulfinyl, C1 -C6 alkylsulfonyl, amino, C1-C6 alkylamino, diC1-C6 Alkylamino, sulfonamide, C1-C6 alkoxycarbonyl, carboxyl syl, halogen, hydroxyl, nitro, cyano, azide, phenyl or ben represents zyloxy, and R4 is hydrogen, or a straight chain or branched chain having 1 to 6 carbon atoms. represents a branched saturated or unsaturated aliphatic group] dibenzo[b,e]aze Pin derivatives, their tautomers, enantiomers, diastereomers and physiologically Compatible salts. 2. R1 to R3 are hydrogen, C1-C3 alkyl, C2-C4 alkenyl, C2-C 4 alkynyl, C1-C3 alkoxy, C1-C2 alkylmercapto, C1- C3 alkylamino, C1-C2 alkoxycarbonyl, amino, halogen, hydrogen Dibe according to claim 1, characterized in that it represents droxyl, cyano or azide. Nzo[b,e]azepine derivatives. 3. R4 is hydrogen, C1-C2 alkyl, C2-C4 alkenyl or C2-C4 Dibenzo[b,e] according to claim 1 or 2, characterized in that it represents alkynyl. ]Azepine derivative. 4. Preparation of dibenzo[b,e]azepine derivatives of formula I according to claim 1, 2 or 3. A manufacturing method, a) Formula II: ▲There are mathematical formulas, chemical formulas, tables, etc.▼(II) [In the formula, A, X, n and R1 to R 4 has the above meaning and Y represents a reactive group]; or b ) Formula III: ▲There are mathematical formulas, chemical formulas, tables, etc.▼(III) [In the formula, A, X, n, R1 to R4 and Y has the abovementioned meaning] with separation of HY; or c) Formula IV: ▲There are mathematical formulas, chemical formulas, tables, etc.▼(IV) [In the formula, A, X and R1 to R4 are having the above meaning] and the compound of formula V: Y'-(CH2)n-Y''(V) [wherein n has the above meaning and Y' and Y'' are the same or different, and has the meaning of Y, with the separation of HY' and HY''. or d) formula VI: ▲There are mathematical formulas, chemical formulas, tables, etc.▼(VI) [In the formula, A, X, n and R1 to R 4 has the above meaning and Z represents a reactive group]; or or e) one or more of the n CH2 groups is replaced with CO or a derivative thereof. converting the compound of formula (I) which has been converted into a compound of formula I by reduction; and, optionally, subsequently converting the compound of formula I into other compounds of formula I falling within the scope of the claims. titration with a pharmacologically compatible acid or base, if desired. A method characterized by converting the salt into salt. 5. At least one dibenzo[b,e]a of formula I according to claims 1, 2 or 3. Pharmaceutical compositions containing a zepine derivative and customary carriers or auxiliary substances. 6. Preparing medicines for the treatment of diseases caused by viruses or retroviruses dibenzo[b,e]azepine derivatives of formula I according to claim 1, 2 or 3 for use.